TY - JOUR
T1 - Mutations in a novel isoform of TRIOBP that encodes a filamentous-actin binding protein are responsible for DFNB28 recessive nonsyndromic hearing loss
AU - Shahin, Hashem
AU - Walsh, Tom
AU - Sobe, Tama
AU - Abu Sa'ed, Judeh
AU - Abu Rayan, Amal
AU - Lynch, Eric D.
AU - Lee, Ming K.
AU - Avraham, Karen B.
AU - King, Mary Claire
AU - Kanaan, Moein
N1 - Funding Information:
We thank the students, families, and staff of the Palestinian schools for children with hearing loss, for their enthusiastic participation. We thank Katja Seipel and Michel Streuli for TARA.27 and TARA.397 antibodies to TRIOBP, Dr. Wa’el Salhab for clinical examinations, and Amiel Dror for figures. H.S. is supported by the Canadian International Scientific Exchange Program (CISEPO). This project was supported by NIH grant R01 DC005641. This work was performed by H.S. in partial fulfillment of the requirements for a Ph.D. degree, Sackler Faculty of Medicine, Tel Aviv University.
PY - 2006/1
Y1 - 2006/1
N2 - In a large consanguineous Palestinian kindred, we previously mapped DFNB28-a locus associated with recessively inherited, prelingual, profound sensorineural hearing impairment-to chromosome 22q13.1. We report here that mutations in a novel 218-kDa isoform of TRIOBP (TRIO and filamentous actin [F-actin] binding protein) are associated with DFNB28 hearing loss in a total of nine Palestinian families. Two nonsense mutations (R347X and Q581X) truncate the protein, and a potentially deleterious missense mutation (G1019R) occurs in a conserved motif in a putative SH3-binding domain. In seven families, 27 deaf individuals are homozygous for one of the nonsense mutations; in two other families, 3 deaf individuals are compound heterozygous for the two nonsense mutations or for Q581X and G1019R. The novel long isoform of TRIOBP has a restricted expression profile, including cochlea, retina, and fetal brain, whereas the original short isoform is widely expressed. Antibodies to TRIOBP reveal expression in sensory cells of the inner ear and colocalization with F-actin along the length of the stereocilia.
AB - In a large consanguineous Palestinian kindred, we previously mapped DFNB28-a locus associated with recessively inherited, prelingual, profound sensorineural hearing impairment-to chromosome 22q13.1. We report here that mutations in a novel 218-kDa isoform of TRIOBP (TRIO and filamentous actin [F-actin] binding protein) are associated with DFNB28 hearing loss in a total of nine Palestinian families. Two nonsense mutations (R347X and Q581X) truncate the protein, and a potentially deleterious missense mutation (G1019R) occurs in a conserved motif in a putative SH3-binding domain. In seven families, 27 deaf individuals are homozygous for one of the nonsense mutations; in two other families, 3 deaf individuals are compound heterozygous for the two nonsense mutations or for Q581X and G1019R. The novel long isoform of TRIOBP has a restricted expression profile, including cochlea, retina, and fetal brain, whereas the original short isoform is widely expressed. Antibodies to TRIOBP reveal expression in sensory cells of the inner ear and colocalization with F-actin along the length of the stereocilia.
UR - http://www.scopus.com/inward/record.url?scp=29244481972&partnerID=8YFLogxK
U2 - 10.1086/499495
DO - 10.1086/499495
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AN - SCOPUS:29244481972
SN - 0002-9297
VL - 78
SP - 144
EP - 152
JO - American Journal of Human Genetics
JF - American Journal of Human Genetics
IS - 1
ER -